Adrenocorticotropin resistance syndromes.

[triple a syndrome]

Familial glucocorticoid deficiency (FGD ) and triple A syndrome belong to a rare group of autosomal recessive disorders characterized by adrenocorticotropin (ACTH ) insensitivity . Unlike triple A syndrome which presents a range of clinical features , FGD is solely characterized by glucocorticoid deficiency . ACTH regulates steroid biosynthesis in the adrenal cortex by exerting its effects via the ACTH receptor (melanocortin- 2 receptor , MC 2 R ). In FGD , mutations in the MC 2 R account for only approximately 25 % of cases (FGD type 1 ). The inability to express a functional MC 2 R in non-adrenal cell lines had implied the presence of an adrenal specific accessory factor (s ), essential for MC 2 R expression . More recently , this factor was identified as melanocortin receptor accessory protein (MRAP ). Mutations in MRAP account for 20 % of cases (FGD type 2 ). Like the receptor activity-modifying proteins (RAMPs ) and receptor transporter proteins (RTPs ), which are well-characterized accessory proteins for G-protein-coupled receptors (GPCRs ), MRAP is a small single transmembrane domain protein . MRAP is essential for the functional expression of the MC 2 R . About 55 % of FGD cases have no identifiable gene defect , implying the involvement of additional genes . This chapter briefly describes the clinical and biochemical features of ACTH resistance syndromes . However , we will focus on the recent progress made towards understanding the molecular defect underlying these conditions , in particular the interaction of MC 2 R and MRAP .